saquinavir

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CAS: 127779-20-8
MF: C38H50N6O5
MW: 670.8408
Synonyms: saquinavir

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Bo Liu

The University of Science and Technology of China
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Charles S. Craik

University of California
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Lei Wang

University of California San Francisco
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David I. Schuster

New York University
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Gail E. Fanucci

University of Florida
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Co-reporter: Ian Mitchelle S. de Vera, Mandy E. Blackburn, and Gail E. Fanucci
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Publication Date(Web):September 25, 2012
DOI: 10.1021/bi301010z
Inhibitor-induced conformational ensemble shifts in a multidrug resistant HIV-1 protease variant, MDR769, are characterized by site-directed spin labeling double electron–electron resonance spectroscopy. For MDR769 compared to the native enzyme, changes in inhibitor IC50 values are related to a parameter defined as |ΔC|, which is the relative change in the inhibitor-induced shift to the closed state. Specifically, a linear correlation is found between |ΔC| and the magnitude of the change in IC50, provided that inhibitor binding is not too weak. Moreover, inhibitors that exhibit MDR769 resistance no longer induce a strong shift to a closed conformational ensemble as seen previously in the native enzyme.

Adrian E. Roitberg

University of Florida
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Chia-en A. Chang

University of California
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Ashok Mulchandani

University of California, Riverside
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Wonhwa Cho

University of Illinois at Chicago
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Arieh Warshel

University of Southern California
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